The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement

Human RNase 6 is a cationic secreted protein that belongs to the RNase A superfamily. Its expression is induced in neutrophils and monocytes upon bacterial infection, suggesting a role in host defence. We present here the crystal structure of RNase 6 obtained at 1.72 Å (1 Å=0.1 nm) resolution, which...

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Autores principales: Prats-Ejarque, Guillem, Arranz-Trullén, Javier, Blanco, Jose A., Pulido, David, Nogués, M. Victòria, Moussaoui, Mohammed, Boix, Ester
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Portland Press Ltd. 2016
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4888456/
https://www.ncbi.nlm.nih.gov/pubmed/27013146
http://dx.doi.org/10.1042/BCJ20160245
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author Prats-Ejarque, Guillem
Arranz-Trullén, Javier
Blanco, Jose A.
Pulido, David
Nogués, M. Victòria
Moussaoui, Mohammed
Boix, Ester
author_facet Prats-Ejarque, Guillem
Arranz-Trullén, Javier
Blanco, Jose A.
Pulido, David
Nogués, M. Victòria
Moussaoui, Mohammed
Boix, Ester
author_sort Prats-Ejarque, Guillem
collection PubMed
description Human RNase 6 is a cationic secreted protein that belongs to the RNase A superfamily. Its expression is induced in neutrophils and monocytes upon bacterial infection, suggesting a role in host defence. We present here the crystal structure of RNase 6 obtained at 1.72 Å (1 Å=0.1 nm) resolution, which is the first report for the protein 3D structure and thereby setting the basis for functional studies. The structure shows an overall kidney-shaped globular fold shared with the other known family members. Three sulfate anions bound to RNase 6 were found, interacting with residues at the main active site (His(15), His(122) and Gln(14)) and cationic surface-exposed residues (His(36), His(39), Arg(66) and His(67)). Kinetic characterization, together with prediction of protein–nucleotide complexes by molecular dynamics, was applied to analyse the RNase 6 substrate nitrogenous base and phosphate selectivity. Our results reveal that, although RNase 6 is a moderate catalyst in comparison with the pancreatic RNase type, its structure includes lineage-specific features that facilitate its activity towards polymeric nucleotide substrates. In particular, enzyme interactions at the substrate 5′ end can provide an endonuclease-type cleavage pattern. Interestingly, the RNase 6 crystal structure revealed a novel secondary active site conformed by the His(36)–His(39) dyad that facilitates the polynucleotide substrate catalysis.
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spelling pubmed-48884562016-06-08 The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement Prats-Ejarque, Guillem Arranz-Trullén, Javier Blanco, Jose A. Pulido, David Nogués, M. Victòria Moussaoui, Mohammed Boix, Ester Biochem J Research Articles Human RNase 6 is a cationic secreted protein that belongs to the RNase A superfamily. Its expression is induced in neutrophils and monocytes upon bacterial infection, suggesting a role in host defence. We present here the crystal structure of RNase 6 obtained at 1.72 Å (1 Å=0.1 nm) resolution, which is the first report for the protein 3D structure and thereby setting the basis for functional studies. The structure shows an overall kidney-shaped globular fold shared with the other known family members. Three sulfate anions bound to RNase 6 were found, interacting with residues at the main active site (His(15), His(122) and Gln(14)) and cationic surface-exposed residues (His(36), His(39), Arg(66) and His(67)). Kinetic characterization, together with prediction of protein–nucleotide complexes by molecular dynamics, was applied to analyse the RNase 6 substrate nitrogenous base and phosphate selectivity. Our results reveal that, although RNase 6 is a moderate catalyst in comparison with the pancreatic RNase type, its structure includes lineage-specific features that facilitate its activity towards polymeric nucleotide substrates. In particular, enzyme interactions at the substrate 5′ end can provide an endonuclease-type cleavage pattern. Interestingly, the RNase 6 crystal structure revealed a novel secondary active site conformed by the His(36)–His(39) dyad that facilitates the polynucleotide substrate catalysis. Portland Press Ltd. 2016-05-27 2016-06-01 /pmc/articles/PMC4888456/ /pubmed/27013146 http://dx.doi.org/10.1042/BCJ20160245 Text en © 2016 The Author(s). published by Portland Press Limited on behalf of the Biochemical Society
spellingShingle Research Articles
Prats-Ejarque, Guillem
Arranz-Trullén, Javier
Blanco, Jose A.
Pulido, David
Nogués, M. Victòria
Moussaoui, Mohammed
Boix, Ester
The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement
title The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement
title_full The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement
title_fullStr The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement
title_full_unstemmed The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement
title_short The first crystal structure of human RNase 6 reveals a novel substrate-binding and cleavage site arrangement
title_sort first crystal structure of human rnase 6 reveals a novel substrate-binding and cleavage site arrangement
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4888456/
https://www.ncbi.nlm.nih.gov/pubmed/27013146
http://dx.doi.org/10.1042/BCJ20160245
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